Effect of NXY‐059 on infarct volume after transient or permanent middle cerebral artery occlusion in the rat; studies on dose, plasma concentration and therapeutic time window

Sydserff, S G; Borelli, A; Green, A R; Cross, A.J.

doi:10.1038/sj.bjp.0704449

Cited by 148 publications

(127 citation statements)

References 39 publications

(59 reference statements)

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“…Even when started at 3 h of recirculation (i.e., 5 h after the onset of ischemia), neurologic deficits were still improved and infarct volume was still reduced by approximately two-thirds. Other workers confirmed these effects in similar models (Sydserff et al, 2002) Neuroprotective effects were also described in rat models of permanent MCA occlusion: In one such study, higher-dose NXY-059 treatment begun at 5 min after onset of permanent MCA occlusion in spontaneously hypertensive (SHR) rats led to a 36% reduction in cortical infarct volume ). In another permanent-occlusion model in rats, 44% infarct reduction was observed even when treatment was initiated at 4 h after stroke onset (Sydserff et al, 2002).…”

Section: Magnesiummentioning

confidence: 74%

Neuroprotection for ischemic stroke: Past, present and future

2008

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Neuroprotection for ischemic stroke refers to strategies, applied singly or in combination, that antagonize the injurious biochemical and molecular events that eventuate in irreversible ischemic injury. There has been a recent explosion of interest in this field, with over 1000 experimental papers and over 400 clinical articles appearing within the past 6 years. These studies, in turn, are the outgrowth of three decades of investigative work to define the multiple mechanisms and mediators of ischemic brain injury, which constitute potential targets of neuroprotection. Rigorously conducted experimental studies in animal models of brain ischemia provide incontrovertible proof-of-principle that high-grade protection of the ischemic brain is an achievable goal. Nonetheless, many agents have been brought to clinical trial without a sufficiently compelling evidence-based pre-clinical foundation. At this writing, around 160 clinical trials of neuroprotection for ischemic stroke have been initiated. Of the approximately 120 completed trials, two-thirds were smaller early-phase safetyfeasibility studies. The remaining one-third were typically larger (>200 subjects) phase II or III trials, but, disappointingly, only fewer than one-half of these administered neuroprotective therapy within the 4-6 hour therapeutic window within which efficacious neuroprotection is considered to be achievable. This fact alone helps to account for the abundance of "failed" trials.This review presents a close survey of the most extensively evaluated neuroprotective agents and classes and considers both the strengths and weakness of the pre-clinical evidence as well as the results and shortcomings of the clinical trials themselves. Among the agent-classes considered are calcium channel blockers; glutamate antagonists; GABA agonists; antioxidants/radical scavengers; phospholipid precursor; nitric oxide signal-transduction down-regulator; leukocyte inhibitors; hemodilution; and a miscellany of other agents. Among promising ongoing efforts, therapeutic hypothermia, high-dose human albumin therapy, and hyperacute magnesium therapy are considered in detail. The potential of combination therapies is highlighted. Issues of clinical-trial funding, the need for improved translational strategies and clinical-trial design, and "thinking outside the box" are emphasized. Part I: Neuroprotection -from Past to the PresentNeuroprotection for ischemic brain injury has emerged only recently as a topic of serious biomedical inquiry. A MEDLINE survey (PubMed, 2007) reveals virtually no publications on this topic until the early 1990's but a remarkable surge in publications over the past 10 years Correspondence and reprint requests to:

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Section: Magnesiummentioning

confidence: 74%

Neuroprotection for ischemic stroke: Past, present and future

2008

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“…In contrast, NXY-059 was ineffective at a concentration (300 mmol/L), which both markedly exceeds that required in plasma for a maximum neuroprotective effect in animal models of stroke in vivo (150 mmol/L; Sydserff et al, 2002) and is also greater than the targeted steady-state concentration (260 mmol/L) in the recent Phase III trials of NXY-059 in acute stroke (Lees et al, 2006). Direct nitration of amino acid tyrosine by peroxynitrite was also abolished by the antioxidant cocktail, but was unaffected by NXY-059.…”

Section: Discussionmentioning

confidence: 97%

“…a-Phenyl-N-tert-butylnitrone (PBN) has been extensively studied in both permanent and transient focal ischaemia models in rats, and its close congener 2-sulphophenyl-N-tertbutylnitrone (S-PBN) is also an established neuroprotective agent . Disodium 2,4-sulphophenyl-N-tert-butylnitrone (NXY-059) is another derivative of PBN that has showed an impressive neuroprotective profile in both rodent and primate models of acute ischaemic stroke (Sydserff et al, 2002;Marshall et al, 2003;Green and Ashwood, 2005). Surprisingly, evidence for nitrones having cytoproprotective activity in vitro is sparse.…”

Section: Introductionmentioning

confidence: 99%

The Nitrone Disodium 2,4-Sulphophenyl-N-Tert-Butylnitrone is Without Cytoprotective Effect on Sodium Nitroprusside-Induced Cell Death in N1E-115 Neuroblastoma Cells in vitro

Hainsworth

Bhuiyan

Green

2007

J Cereb Blood Flow Metab

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Disodium 2,4-sulphophenyl-N-tert-butylnitrone (NXY-059) is a novel free radical-trapping compound that is neuroprotective in both rodent and primate models of acute ischaemic stroke. Neuroprotection in vitro by NXY-059 has not been reported previously, and we have now investigated whether such an effect can be detected using a simple cell culture model of neurotoxicity. Neuron-like cells of the neuroblastoma-derived clonal cell line N1E-115 were exposed to the free radical-generating agent sodium nitroprusside (SNP), which produced a concentration-dependent reduction in mitochondrial complex II activity 24 h later (EC 50 approximately 100 micromolar). Cell death induced by SNP (100 micromolar), assessed either by an increased proportion of apoptotic nuclear morphology or by mitochondrial complex II activity, was inhibited by a cocktail of known antioxidants (ascorbate, reduced glutathione, and dithiothreitol, all at 100 micromolar) but not by NXY-059 at a concentration known to be neuroprotective in vivo (300 micromolar). Disodium 2,4-sulphophenyl-N-tert-butylnitrone was also without effect on H 2 O 2 -mediated cytotoxicity. These results support recent data suggesting that in vivo NXY-059 probably acts at the neurovascular unit rather than at an intracellular site as a neuroprotective agent.

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“…Several nitrone free radical-trapping agents (i.e., spin-trap agents) have demonstrated neuroprotection in rodent models of both transient and permanent focal ischemia [111,112]. NXY-059 (disodium 4-[(tert-butylimino) methyl] benzene-1,3-disulfonate N-oxide) is a novel nitrone-based compound that has free radical-trapping properties.…”

Section: Red Blood Cell Breakdown and Toxic Breakdown Products: Free mentioning

confidence: 99%

Treatment Targets in Intracerebral Hemorrhage

Sangha

Gonzales

2011

Neurotherapeutics

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Intracerebral hemorrhage (ICH) imparts a higher mortality and morbidity than ischemic stroke. The therapeutic interventions that are currently available focus mainly on supportive care and secondary prevention. There is a paucity of evidence to support any one acute intervention that improves functional outcome. This chapter highlights current treatment targets for ICH based on the pathophysiology of the disease.

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Effect of NXY‐059 on infarct volume after transient or permanent middle cerebral artery occlusion in the rat; studies on dose, plasma concentration and therapeutic time window

Cited by 148 publications

References 39 publications

Neuroprotection for ischemic stroke: Past, present and future

Neuroprotection for ischemic stroke: Past, present and future

The Nitrone Disodium 2,4-Sulphophenyl-N-Tert-Butylnitrone is Without Cytoprotective Effect on Sodium Nitroprusside-Induced Cell Death in N1E-115 Neuroblastoma Cells in vitro

Treatment Targets in Intracerebral Hemorrhage

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